Cell Reports (Jul 2023)

DENND2B activates Rab35 at the intercellular bridge, regulating cytokinetic abscission and tetraploidy

  • Rahul Kumar,
  • Vincent Francis,
  • Maria S. Ioannou,
  • Adriana Aguila,
  • Maleeha Khan,
  • Emily Banks,
  • Gopinath Kulasekaran,
  • Peter S. McPherson

Journal volume & issue
Vol. 42, no. 7
p. 112795

Abstract

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Summary: Cytokinesis relies on membrane trafficking pathways regulated by Rabs and guanine nucleotide exchange factors (GEFs). During cytokinesis, the intercellular cytokinetic bridge (ICB) connecting daughter cells undergoes abscission, which requires actin depolymerization. Rab35 recruits MICAL1 to oxidize and depolymerize actin filaments. We show that DENND2B, a protein linked to cancer and congenital disorders, functions as a Rab35 GEF, recruiting and activating Rab35 at the ICB. DENND2B’s N-terminal region also interacts with an active form of Rab35, suggesting that DENND2B is both a Rab35 GEF and effector. Knockdown of DENND2B delays abscission, leading to multinucleated cells and filamentous actin (F-actin) accumulation at the ICB, impairing recruitment of ESCRT-III at the abscission site. Additionally, F-actin accumulation triggers the formation of a chromatin bridge, activating the NoCut/abscission checkpoint, and DENND2B knockdown activates Aurora B kinase, a hallmark of checkpoint activation. Thus, our study identifies DENND2B as a crucial player in cytokinetic abscission.

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